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PIPK1b regulates E-cadherin endocytosis in polarized breast cancer cells and promotes a switch to a migratory phenotype

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dc.contributor.author Azhunussova, A.
dc.contributor.author Shayakhmetov, Y.
dc.contributor.author Chao, W. T.
dc.contributor.author Kunz, J.
dc.date.accessioned 2015-10-26T08:30:24Z
dc.date.available 2015-10-26T08:30:24Z
dc.date.issued 2014
dc.identifier.isbn 9786018046728
dc.identifier.uri http://nur.nu.edu.kz/handle/123456789/458
dc.description.abstract The endocytosis, degradation, and recycling of cadherins is crucial for the dynamic regulation of adherens junctions and the control of cell-cell adhesion during tissue formation and in many pathological conditions. In order to allow for dynamic changes in intercellular adhesion, adherens junctions assemble and disassemble in a continuous fashion. A key mechanism for modulating adhesion strength is the adjustment of the cell surface levels of E-cadherin, the major component of adherens junctions. E-cadherin endocytosis, often accompanied by its degradation, has been observed in many developmental and disease processes and accounts for more rapid changes in adhesion strength that can occur independently of the transcriptional regulation of E-cadherin. However, the molecular mechanisms underlying E-cadherin endocytosis and recycling remain incompletely understood. ru_RU
dc.language.iso en ru_RU
dc.publisher Nazarbayev University ru_RU
dc.subject endocytosis ru_RU
dc.subject degradation ru_RU
dc.subject cadherins ru_RU
dc.subject dynamic regulation ru_RU
dc.subject pathological conditions ru_RU
dc.subject migratory phenotype ru_RU
dc.title PIPK1b regulates E-cadherin endocytosis in polarized breast cancer cells and promotes a switch to a migratory phenotype ru_RU
dc.type Abstract ru_RU


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